Disease Models & Mechanisms (Nov 2016)

Restoration of mutant bestrophin-1 expression, localisation and function in a polarised epithelial cell model

  • Carolina Uggenti,
  • Kit Briant,
  • Anne-Kathrin Streit,
  • Steven Thomson,
  • Yee Hui Koay,
  • Richard A. Baines,
  • Eileithyia Swanton,
  • Forbes D. Manson

DOI
https://doi.org/10.1242/dmm.024216
Journal volume & issue
Vol. 9, no. 11
pp. 1317 – 1328

Abstract

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Autosomal recessive bestrophinopathy (ARB) is a retinopathy caused by mutations in the bestrophin-1 protein, which is thought to function as a Ca2+-gated Cl− channel in the basolateral surface of the retinal pigment epithelium (RPE). Using a stably transfected polarised epithelial cell model, we show that four ARB mutant bestrophin-1 proteins were mislocalised and subjected to proteasomal degradation. In contrast to the wild-type bestrophin-1, each of the four mutant proteins also failed to conduct Cl− ions in transiently transfected cells as determined by whole-cell patch clamp. We demonstrate that a combination of two clinically approved drugs, bortezomib and 4-phenylbutyrate (4PBA), successfully restored the expression and localisation of all four ARB mutant bestrophin-1 proteins. Importantly, the Cl− conductance function of each of the mutant bestrophin-1 proteins was fully restored to that of wild-type bestrophin-1 by treatment of cells with 4PBA alone. The functional rescue achieved with 4PBA is significant because it suggests that this drug, which is already approved for long-term use in infants and adults, might represent a promising therapy for the treatment of ARB and other bestrophinopathies resulting from missense mutations in BEST1.

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